Search Result Details | circRNADisease v3.0

circRNA basic information

circBase ID:	-
Name:	hsa_circ_CDYL
Synonym:	circCDYL / Circular RNA CDYL
Host Gene:	CDYL
Genomic location(hg19):	-
Genomic location(hg38):	-
Subcellular localization:	cytoplasm

Disease basic information

MONDO ID:	0021063
MONDO name:	malignant colon neoplasm
Disease details:	colon cancer
Disease DO ID:	219
Disease MeSH ID:	-
Disease NCIt ID:	C9242
Disease ICD11 ID:	1265576634
Disease OMIM ID:	-
Species:	Human
Species details:	Homo sapiens
Tissue specimen:	colon cancer tissues; paired surrounding normal tissues
Cell lines:	SW480; SW620
In vivo animal model:	-

circRNA-disease information

Expression pattern:	DN
Associated gene:	PTEN, PI3K, AKT, JAK2, STAT5, c-Myc, cyclin D1, p53, caspase-3, PARP
Associated microRNA:	miR-150-5p
Biological function:	circCDYL suppresses colon cancer cell viability, colony formation, migration and invasion, and promotes apoptosis.
Molecular mechanism:	circCDYL represses miR-150-5p, increases PTEN, and blocks PI3K/AKT and JAK/STAT signaling cascades to exert an antitumor role in colon cancer cells.
Biological pathway or process:	PI3K/AKT (inhibits); JAK/STAT (inhibits); proliferation (inhibits); migration (inhibits); invasion (inhibits); apoptosis (promotes); ceRNA regulation (other)
Detected method:	Q
Validation methods:	RT-qPCR; Clinical Sample Validation; Transfection; CCK8; Colony Formation Assay; Annexin V/PI Flow Cytometry; Transwell Assay; Western Blot
Clinical significance:	circCDYL is decreased in colon cancer tissues and was considered a promising candidate for colon cancers.
Description:	circCDYL was down-regulated in colon cancer tissues compared with adjacent tissues. Its overexpression inhibited colon cancer cell growth, migration and invasion, promoted apoptosis, and acted through repression of miR-150-5p with downstream blockade of PI3K/AKT and JAK/STAT signaling.
Confidence score:	0.5434

Other information

Title:	circCDYL/microRNA-105-5p participates in modulating growth and migration of colon cancer cells.
Journal:	General physiology and biophysics
Published:	2019
PubMed ID:	31829306
Study type:	combined biological and clinical study
Data availability:	-
Code availability:	-